Abstract

Enzymes perform many of the most vital functions in our cells and tissues and are the targets of numerous transformative medicines. Considering the importance of enzymes in health and disease, it is both provocative and humbling to realize that the human proteome contains a huge number of uncharacterized enzymes. Assigning functions to these enzymes represents a grand challenge for researchers in the post-genomic era. To achieve this goal, selective pharmacological tools to perturb enzymes in living systems are needed. A pressing question, however, arises: how can one rapidly and systematically discover inhibitors for poorly characterized enzymes? Over the past decade, our lab has pioneered the development and application of an innovative chemical proteomic solution to this problem termed activity-based protein profiling (ABPP). The objective of this application is to use ABPP to discover potent, selective, and in vivo-active inhibitors for serine hydrolases (SHs), which are a large and diverse enzyme class that represents ~1% of all human proteins. SHs play critical roles in human physiology and disease and are targeted by several approved drugs. Despite their biological and biomedical importance, most SHs, including many with genetic links to human disease, lack inhibitors and consequently remain poorly understood with regards to their physiologic substrates and functions. In this this competitive renewal project, we will focus on inhibiting and functionally characterizing SHs with established or emergent roles in neurobiological processes. During the previous grant period, we created an efficient ABPP platform for SH inhibitor discovery and optimization that has already yielded selective and in vivo-active inhibitors for several SHs, as well as lead inhibitors for many additional enzymes. In most cases, these compounds represent the first pharmacological probes for studying their SH targets in living systems and are in widespread use by the biology research community. In this application, we propose to use a multidisciplinary research program that integrates ABPP with chemical synthesis, lipidomics, mouse genetics, and cell and animal pharmacology to selectively inhibit and functionally characterize: 1) SHs that regulate the biosynthesis of the endocannabinoid class of lipid transmitters in the nervous system (Specific Aim 1), and 2) SHs and SH pathways with genetic links to human neurological disorders (Specific Aim 2). We have enlisted a strong set of biology collaborators who will apply our optimized inhibitors to mouse models of nervous system function and disease. The inhibitors generated and knowledge gained herein should greatly advance our understanding of the functions of SHs and SH pathways, enabling the identification of drug targets to treat human neurological diseases.

Public Health Relevance

A large fraction of drugs used to treat human disease inhibit enzymes. The human genome encodes a huge number of uncharacterized enzymes, many of which have clear genetic associations with disease. The goal of this application is to develop inhibitors for and functionally characterize serine hydrolase enzymes to identify new targets and pathways for treating neurological disorders.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Drug Abuse (NIDA)
Type
Research Project (R01)
Project #
5R01DA033760-08
Application #
9673095
Study Section
Synthetic and Biological Chemistry B Study Section (SBCB)
Program Officer
Rapaka, Rao
Project Start
2012-04-01
Project End
2022-03-31
Budget Start
2019-04-01
Budget End
2020-03-31
Support Year
8
Fiscal Year
2019
Total Cost
Indirect Cost

  Institution

Name
Scripps Research Institute
Department
Type
DUNS #
781613492
City
La Jolla
State
CA
Country
United States
Zip Code
92037

  Publications

Inloes, Jordon M; Jing, Hui; Cravatt, Benjamin F (2018) The Spastic Paraplegia-Associated Phospholipase DDHD1 Is a Primary Brain Phosphatidylinositol Lipase. Biochemistry 57:5759-5767
Cheng, Ran; Mori, Wakana; Ma, Longle et al. (2018) In Vitro and in Vivo Evaluation of 11C-Labeled Azetidinecarboxylates for Imaging Monoacylglycerol Lipase by PET Imaging Studies. J Med Chem 61:2278-2291
Inloes, Jordon M; Kiosses, William B; Wang, Huajin et al. (2018) Functional Contribution of the Spastic Paraplegia-Related Triglyceride Hydrolase DDHD2 to the Formation and Content of Lipid Droplets. Biochemistry 57:827-838
Ogasawara, Daisuke; Ichu, Taka-Aki; Vartabedian, Vincent F et al. (2018) Selective blockade of the lyso-PS lipase ABHD12 stimulates immune responses in vivo. Nat Chem Biol 14:1099-1108
Curry, Zachary A; Wilkerson, Jenny L; Bagdas, Deniz et al. (2018) Monoacylglycerol Lipase Inhibitors Reverse Paclitaxel-Induced Nociceptive Behavior and Proinflammatory Markers in a Mouse Model of Chemotherapy-Induced Neuropathy. J Pharmacol Exp Ther 366:169-183
Suciu, Radu M; Cognetta 3rd, Armand B; Potter, Zachary E et al. (2018) Selective Irreversible Inhibitors of the Wnt-Deacylating Enzyme NOTUM Developed by Activity-Based Protein Profiling. ACS Med Chem Lett 9:563-568
Owens, Robert A; Mustafa, Mohammed A; Ignatowska-Jankowska, Bogna M et al. (2017) Inhibition of the endocannabinoid-regulating enzyme monoacylglycerol lipase elicits a CB1 receptor-mediated discriminative stimulus in mice. Neuropharmacology 125:80-86
Yun, Bogeon; Lee, HeeJung; Powell, Roger et al. (2017) Regulation of calcium release from the endoplasmic reticulum by the serine hydrolase ABHD2. Biochem Biophys Res Commun 490:1226-1231
Tan, Joanne; Cognetta Iii, Armand B; Diaz, Diego B et al. (2017) Multicomponent mapping of boron chemotypes furnishes selective enzyme inhibitors. Nat Commun 8:1760
van Esbroeck, Annelot C M; Janssen, Antonius P A; Cognetta 3rd, Armand B et al. (2017) Activity-based protein profiling reveals off-target proteins of the FAAH inhibitor BIA 10-2474. Science 356:1084-1087

Showing the most recent 10 out of 48 publications